This was a retrospective observational study that included patients treated at the University Hospital of Nice, France, over a period spanning from January 1^st 2015 au June 30^th 2022. Subjects aged 17 years and above were identified via a database search for antiphospholipid positivity, and those meeting the 2006 Sydney classification criteria for APS were selected for the study (2) ( Supplementary Data , Supplementary Table S2 ). Patients with duplicate and/or missing data – as well as those that lacked an immunological work-up with ANA – were excluded from the study even if APS criteria were met.

Catastrophic antiphospholipid syndrome (CAPS) was defined according to Asherson et al. (16). Whereas, “microvascular involvement” referred to livedo racemosa, livedoid vasculopathy, aPL nephropathy and/or pulmonary hemorrhage based on the latest classification criteria (3). Diagnoses of systemic lupus erythematosus (SLE) were those made in the clinical setting and were retrospectively required to meet any of the classification criteria for the disease (17). ANA were considered positive for titres above 1/160 (expressed as “≥1/160” in the manuscript). Immunological markers with their ranges are presented in the Supplementary Data section ( Supplementary Table S3 ).

Data were collected from patients’ digital medical files and included findings such as demographics, clinical characteristics (including comorbidities, initial symptoms, microvascular involvement and cardio- and cerebro-vascular risk factors) and laboratory workup. Focus was given to hematological and immunological features such as: LA, aCL and aβ2-GP.I with their IgM and IgG antibody isotypes, platelet counts, creatinine and kidney function, ANA and complement function tests. The estimated glomerular filtration rate (eGFR) was based on the Modification of Diet in Renal Disease Study Group (MDRD) method (18). Immuno-assays with their associated cut-off values are provided as Supplementary Data ( Supplementary Table S3 ).

“Double-positive aPL” was defined as the positivity of any combination of two aPL biomarkers irrespective of immunoglobulin isotype for aCL and/or aβ2-GP.I, whereas “triple positivity” referred to the presence of all three aPL biomarkers (irrespective of immunoglobulin isotype).

Based on previous studies (6–11) ( Supplementary Data , Supplementary Table S4 ), clinical relevance and the recent 2023 ACR/EULAR classification criteria for APS (3), we chose the following 24 categories for the hierarchical cluster analysis: age of >50 years, gender, arterial hypertension, diabetes mellitus, dyslipidemia, smoking, obesity, SLE, initial arterial and/or venous thrombotic event, cardiac valve involvement, microvascular involvement, CAPS, obstetric features, LA, IgM and IgG aCL, IgM and IgG aβ2-GP.I, thrombocytopenia <130*10⁹/L, eGFR <60 mL/mn/1.73m², positive ANA, anti-SSA and anti-dsDNA antibody positivity.

Agglomerative unsupervised hierarchical clustering based on the Ward method (for linkage) was performed using the 24 previously stated variables. Euclidian distance was the used metric. The optimal number of clusters was estimated with silhouette scores based on the k-means algorithm for cluster analysis but was also visually assessed with the dendrogram representation of the fusion sequence. Principal coordinates analysis was subsequently used to visualize individual data in a 2-dimensional scatterplot.

Categorical variables were expressed as counts with percentages, and continuous variables as means with their standard deviation (SD). Categorical variables were compared using the Chi² test. ANOVA tests were used to evaluate the difference between multiple means. All analyses were two-tailed and p-values <0.05 were considered statistically significant for comparative studies.

Predictive modelling was performed using the Orange^© data mining software (version 3.35.0) developed by the University of Ljubljana. The JASP^© software (version 0.17.2.1) supported by the University of Amsterdam was used for descriptive and frequentist inference statistical analysis.

Data were anonymized on collection and stored in our institutional electronic repository under the registration number 2023-512 as required by, and in compliance with, French Data Protection Authority (Commission Nationale de l’Informatique et des Libertés) guidelines. In accordance with French law, due to its retrospective nature, this study did not require the validation of an Ethics Committee.

Over the 90-month study period, 174 patients – that were not only diagnosed with APS but for whom ANA were also performed – were included in the hierarchical analysis ( Figure 1 ). Demographics, clinical and biological features at diagnosis are provided in Table 1 .

Antibody titres for aCL and/or aβ2-GP.I (at baseline) were not significantly different between the 4 clusters based on ANOVA testing.

The k-means silhouette score algorithm was able to identify an optimal choice of 4 clusters. These 4 clusters were also visually individualized on the dendrogram ( Figures 2 , 3 ). Incomplete data were estimated to be less than 0.1%.

Taken independently, positive ANA were associated with relapse in the overall cohort of APS patients (p<0.01), with a likelihood ratio (LR) of 12.09. Anti-dsDNA and anti-SSA positivity were also found to be associated with relapse with, respectively, LR of 4.166 (p=0.041) and 3.892 (p=0.048). Patients from cluster 4 presented with the highest number of relapses, whether arterial or venous, compared to the three other groups ( Table 2 ), regardless of anti-dsDNA and anti-SSA antibody-positivity (p=1 and p=0.740, respectively). Arterial thrombosis was more frequent in ANA-positive patients ( Table 2 ).

Patients with cardiovascular disease and aPL positivity are at a high risk of thrombosis as they are likely to have pro-inflammatory endothelial damage in addition to atherosclerosis (5, 20). Such patients also constitute the largest subpopulation amongst subjects with APS as reflected in previous studies (6–11, 19) ( Supplementary Data , Supplementary Table S4 ). It is therefore hardly surprising that our analysis identified this “cardiovascular risk” group that included mostly middle-aged men with arterial thrombosis. Hypertension and medium/high titres of IgG aCL were also identified as risk factors for initial thrombotic events and echoes previous findings (21). However, one should note that risk-assessment of cardiovascular disease, according to the recent classification criteria, might redefine disease status in previously APS-classified patients (3). This implies that the implementation of anticoagulation in patients with a high-risk profile would depend on future relapses and/or criterion from other clinical domains – if such an approach were to be taken literally. Recurrent thrombosis in APS is difficult to assess with rates ranging from 20% to 30% within the first ten years from disease-onset (5, 22, 23). Studies have suggested that thrombotic patterns do not change during the course of the disease (i.e. relapses are either arterial or venous) and thus highlight the importance of an early characterisation of APS phenotypes (6, 12, 24).

Our findings also matched those from previous studies relating to obstetrical events (6, 7, 11). Other authors were not able to individualize such a group due to the variables chosen and/or profile of patients included in the analysis (8, 10). This was particularly the case in the study by Nguyen et al. whose study-population was biased by a high proportion of patients with CAPS (10). Based on our findings, one might argue that the “obstetrical” phenotype is associated with a lesser risk of relapse and, in the absence of macrothrombotic events, antiplatelet aggregating agents may suffice. This observation seems to reflect 2019 EULAR guidelines that recommend low-dose acetylsalicylic acid in non-pregnant women with a history of obstetric APS (after risk/benefit evaluation) as well as in pregnant women with a high-risk aPL profile without a prior history of thrombosis nor pregnancy complications (25). Use of low-dose acetylsalicylic acid could also be considered in patients with clinical “non-criteria” obstetric APS (a grade D recommendation) (25). According to EUROAPS data, thrombotic events occur mostly during pregnancy or the puerperium with only a small subset of patients developing SLE over time (i.e. less than 6%) (26).

Our analysis identified a cluster of patients, mostly female, with VTE and venous relapses (cluster 3). Subjects presented with double or triple positive aPL defining a high-risk profile for two thirds of this subpopulation. This group shared similarities with a frequently described phenotype of patients that have triple-positive aPL and VTE (7–10). Caution should be exercised for treating such patients with DOAC in the absence of phenotype-based clinical trials (27, 28).

Cluster 4 was interesting to analyze since it identified ANA-positive patients with high-risk APS. This particular phenotype has been described in previous studies in groups associating either/or: “non-criteria” features, SLE, cytopenias, microthrombotic events and more frequent arterial thrombosis in mostly female patients (7–11) ( Supplementary Data , Supplementary Table S4 ). ANA-positive APS has been shown to have more “non-criteria” manifestations compared to other forms, an increased frequency of triple-positive aPL and higher rates of relapse (5, 15, 25). In our cohort, thrombosis had the highest rate in this group and occurred despite immunosuppressant drugs, antithrombotic agents and/or hydroxychloroquine intake.

A prior study found that, of the 43% of patients with SLE with positive aPL, only a third were found to have APS (29). The soon-to-be updated EULAR recommendations regarding the management of SLE-associated APS do not, in these aspects, differ from the 2019 guidelines that state that low-dose acetylsalicylic acid can be prescribed in asymptomatic patients with a high-risk aPL profile (30). In light of findings from previous studies and ours, we believe that ANA-positivity should be acknowledged as a risk factor for potential relapses irrespective of a clinical diagnosis of connective tissue disease. Of note, within this cluster, one out of two patients did not present with SLE. This does not imply that anticoagulation is to be started in asymptomatic aPL-positive patients with ANA, but that clinical and biological work-up should focus on microvascular features and/or cytopenias by, for example, assessing for silent APS nephropathy just as one would for lupus nephritis (31). Therefore close monitoring is warranted, especially considering a propensity for CAPS that is associated with a higher mortality rate primarily due to severe cardiac and cerebral involvement (32). Overlapping and associated pro-thrombotic features (including medication) also need to be addressed (19). Furthermore, patients with ANA-positive APS require optimal anticoagulation with vitamin K antagonists although treatment of isolated VTE with DOAC, in this setting, is still a matter of debate (27, 33).

Our study has limitations – the most important of which, being its retrospective nature that may have introduced a selection bias. The latter may have been increased by the deliberate choice of requiring an immunological work-up with ANA and/or the speciality of the physician ordering the analysis. However, this also appears to be one of its strengths since missing data were extremely limited (i.e. less than 0.1%). Another limit of our study relates to the cluster methodology itself, since clinical and biological changes overtime cannot be assessed. Therefore, one cannot exclude the influence of clinical events and treatments on the “re-categorisation” of patients at a given time. However, based on evidence from long-term registry follow-up, changes in disease course do seem exceptional (12, 24). The quality of the clustering process reflects the very stringent inclusion criteria but it does not exempt us from recognizing an unintentional overlap with unreported prothrombotic factors. Our choice of variables for the cluster analysis was established based on previous studies with an emphasis on clinical categories from the recent APS classification criteria (3, 7–11). Our findings are therefore not only in line with previous initiatives but also refine the categorisation of patients with APS; though they may not be extrapolated to different ethnic groups. Our approach chose to focus on clinically relevant events and therefore “asymptomatic patients” were not considered.

The clusters that were identified reflect different clinical presentations and risk profiles. From the clinician’s perspective, patient management could be decided according to the predominant phenotype. For instance, obstetrical APS may only require low-dose acetylsalicylic acid as such individuals qualify as part of a “low risk” group (25). However, attitudes would be different if individuals were to present with: “triple positive” aPL, arterial thrombosis, microvascular involvement, cardiac valve thickening/vegetations (28). From our study, one might add ANA-positivity to these criteria. In such “high risk” cases, full-dose anticoagulation with vitamin K antagonists and/or heparin constitute the corner stone of therapy, in keeping with international guidelines (25). In the case of CAPS, triple therapy associating steroids and plasma exchange to anticoagulation, with rituximab as a first-line immunosuppressor with/without follow-up intravenous immunoglobulins whilst preferring cyclophosphamide in cases with positive ANA (34). We would reserve eculizumab for refractory forms of CAPS, especially in documented complement-mediated thrombotic microangiopathy (35). Similarly, future studies studying anticoagulant and immunosuppressive strategies would require adopting a phenotype-based approach.